Intrauterine enzyme replacement therapies for lysosomal storage disorders: Current developments and promising future prospects

Author:

Herzeg Akos12ORCID,Borges Beltran12,Lianoglou Billie R.12,Gonzalez‐Velez Juan13,Canepa Emma12,Munar Dane1,Young Sarah P.4,Bali Deeksha4,Gelb Michel H.5,Chakraborty Pranesh6,Kishnani Priya S.4,Harmatz Paul7,Cohen Jennifer L.4,MacKenzie Tippi C.127

Affiliation:

1. Center for Maternal‐Fetal Precision Medicine University of California San Francisco California USA

2. Department of Surgery University of California San Francisco California USA

3. Department of Obstetrics and Gynecology and Reproductive Sciences University of California San Francisco California USA

4. Department of Pediatrics Division of Medical Genetics Duke University Durham North Carolina USA

5. Department of Chemistry University of Washington Seattle Washington USA

6. Department of Pediatrics Children's Hospital of Eastern Ontario and University of Ottawa Ottawa Ontario Canada

7. Benioff Children's Hospital University of California San Francisco California USA

Abstract

AbstractLysosomal storage disorders (LSDs) are a group of monogenic condition, with many characterized by an enzyme deficiency leading to the accumulation of an undegraded substrate within the lysosomes. For those LSDs, postnatal enzyme replacement therapy (ERT) represents the standard of care, but this treatment has limitations when administered only postnatally because, at that point, prenatal disease sequelae may be irreversible. Furthermore, most forms of ERT, specifically those administered systemically, are currently unable to access certain tissues, such as the central nervous system (CNS), and furthermore, may initiate an immune response. In utero enzyme replacement therapy (IUERT) is a novel approach to address these challenges evaluated in a first‐in‐human clinical trial for IUERT in LSDs (NCT04532047). IUERT has numerous advantages: in‐utero intervention may prevent early pathology; the CNS can be accessed before the blood‐brain barrier forms; and the unique fetal immune system enables exposure to new proteins with the potential to prevent an immune response and may induce sustained tolerance. However, there are challenges and limitations for any fetal procedure that involves two patients. This article reviews the current state of IUERT for LSDs, including its advantages, limitations, and potential future directions for definitive therapies.

Funder

NIH Clinical Center

Publisher

Wiley

Subject

Genetics (clinical),Obstetrics and Gynecology

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